the touch™ program and risk management pl f th ad i i t ti
TRANSCRIPT
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The TOUCH™ Program and Risk Management Pl f th Ad i i t ti f N t li bPlan for the Administration of Natalizumab:
Updated Safety Results From the Use of Natalizumab in Patients With Relapsing Multiple
Sclerosis and Crohn’s DiseaseSclerosis and Crohn s Disease
Bruce E. Sands1, Gordon Francis2, Gary S. Hogge2, Glyn Belcher3, Mariska Kooijmans3, Richard Kim3, Frances Lynn3, Carmen Bozic3
1Harvard Medical School Massachusetts General Hospital Boston MA1Harvard Medical School, Massachusetts General Hospital, Boston, MA 2Elan Pharmaceuticals, Inc., South San Francisco, CA
3Biogen Idec, Inc., Cambridge, MA
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Disclosures♦ Dr. Bruce Sands is a consultant for Elan
Pharmaceuticals and Biogen Idec, Inc.
♦ Drs. Gordon Francis and Gary S. Hogge are employees of Elan Pharmaceuticals, Inc.
♦ D Gl B l h M i k K ij Ri h d♦ Drs. Glyn Belcher, Mariska Kooijmans, Richard Kim, Frances Lynn, and Carmen Bozic are employees of Biogen Idec, Inc.
♦ TYSABRI is a registered trademark and TOUCH is a trademark of Elan Pharmaceuticals, Inc.
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Background and Objectives♦ Natalizumab, a humanized anti-a4 integrin , g
monoclonal antibody, is indicated for;– Inducing and maintaining clinical response and
remission in adult patients with moderately to severely active Crohn’s disease (CD)
Fc IgG4
severely active Crohn s disease (CD)
• with evidence of inflammation, and
• who have had an inadequate response to, or are unable to tolerate, conventional CD therapies and inhibitors of TNFα
– Relapsing forms of multiple sclerosis (MS)
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Background and Objectives♦ Report the outcomes from ongoing risk management plans p g g g p
to further evaluate the safety of natalizumab– TYSABRI® Outreach: Unified Commitment to Health (TOUCH™)
Prescribing Program
– Investigating Natalizumab Through Further Observational Research d M it i (INFORM) f CDand Monitoring (INFORM) for CD
– TYSABRI Global Observation Program in Safety (TYGRIS) for MS
– Pregnancy registry
♦ Report data on utilization of natalizumab through the end of September 2008
5TOUCH™ Prescribing Program, INFORM,
TYGRIS, Pregnancy Registry♦ TOUCH™ Prescribing Program is mandatory as part of the
FDA Risk Minimization Action Plans (RiskMAP)– Ensure appropriate use of natalizumab and assess the incidence of
serious opportunistic infections, including progressive multifocal leukoencephalopathy (PML), and malignancies
♦ CD INFORM and TYGRIS♦ CD INFORM and TYGRIS– 5 year observational studies of 2000 CD and 5000 MS patients
– Determine incidence and pattern of serious and/or clinically significant infections, including PML, malignancies, & serious adverse events (SAEs), previous medical histories, efficacy
♦ Prospective patient registry to evaluate the outcomes of pregnancy in women with CD or MS
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Update on Estimated Natalizumab Exposure*
48 00050 000 48,000
35,500
30,000
40,000
50,000
tient
s
18,000
9500
370010,000
20,000
Pat
0Total
ExposureCurrently on
Drug12 monthsExposure
18 MonthsExposure
24 MonthsExposure
* Data are as of the end of September 2008 § Includes ~700 clinical trial patients
§
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TOUCH™: Natalizumab Exposure♦ Approximately 3400 prescribing physicians in the pp y p g p y
United States across both indications
♦ 23,989 enrolled patients have received natalizumab treatment (> 99% for MS)
Enrolled patients have received a median of 9– Enrolled patients have received a median of 9 natalizumab infusions (minimum = 1, maximum = 31)
– 313 patients have received natalizumab for CD• 230 patients are currently being treated
• 99 CD patients have received at least 4 infusions
• 83 patients have discontinued therapy (27%)
8TOUCH™: Medication History Over the
Previous 12 months in CD Patients
2%8%
13%
5%
24%
52%
Source: Prior 12-month therapy stated on TOUCH forms received launch-to-date
Multiple Biologics Infliximab AdalimumabNon-Biologics Untreated Unknown
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TYGRIS: Update♦ As of 23 August 2008, 3905 patients have been enrolled
– 72% were female and the mean age was 39 years
– 93% had prior immunomodulatory or immunosuppressant therapy
♦ No unexpected safety issues
♦ Overall SAE incidence was 2.8%– Most common SAEs reported were hypersensitivity reactions (0.4%)
and urinary tract infection (0.2%)
– Incidence of SAEs, including hypersensitivity reactions and , g yp yinfections, was similar to that observed in clinical trials
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Pregnancy Registry: Results♦ 64 women have enrolled prospectivelyp p y♦ Pregnancy outcomes*
– 29 pregnancies currently ongoing– 25 patients delivered 27 healthy babies, including
5 t bi th (2 ith t i )• 5 premature births (2 with twins)– 7 spontaneous abortions– 2 elective terminations
♦ Pregnancy registry continues to actively recruit both CD d MS ti t i i t li bCD and MS patients receiving natalizumab
* One patient declined to continue participation after enrollment with outcome unknown
Data reported are through 23 August 2008
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PML Update♦ There have been 3 confirmed cases of PML in MS patients p
receiving natalizumab in the commercial setting
– 2 cases in EU (31 July 2008) and 1 case in US (29 October 2008)
– All 3 patients underwent plasma exchange and are alive
♦ All cases confirmed based on detection of JC virus (JCV) DNA in CSF in the setting of clinical signs and symptoms and MRI findings consistent with diagnosis of PML
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Algorithm for Diagnosis of PML
Clinical assessment of new neurological symptoms
SUSPEND DOSING
If PML suspected due to clinical presentation and MRI not readily
available, consider CSF to exclude PML prior to MRI
MRI assessment CSF assessmentCannot exclude PML
PML unlikelyJCV not detected
and low clinicalsuspicion
JCV detected
JCV not detected and high clinical
suspicion
* Natalizumab dosing should be restarted only if the diagnosis of PML is excluded and if deemed appropriate for the ongoing treatment of CD. Algorithm is modified based on Kappos L, et al. Lancet Neurol 2007;6:431-441.
Dosing may be resumed*
Treat as PMLRepeat assessment
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Conclusions♦ >48,000 patients worldwide have received natalizumab♦ PML continues to appear to be a rare adverse event
associated with natalizumab treatment– Highlight the importance of the clinical vigilance in monitoring for
early signs and symptoms of PML for early detection
♦ Potential strategies to mitigate the risk of PML include♦ Potential strategies to mitigate the risk of PML include– Identifying patients at risk of developing PML – Monitoring patients to detect PML prior to the development of clinical
signs and symptoms – Treatments to limit disability and prevent death from PML (e.g.,
plasma exchange and antiviral therapies [mefloquine])plasma exchange and antiviral therapies [mefloquine])
♦ Preliminary data from these studies– Support the favorable benefit-risk profile of natalizumab and suggest
a similar safety profile to that seen in previous clinical studies
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Backup Slides
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♦ Male 37 years, diagnosed 2006 in EU with aggressive MS
PML in Post Marketing: Case 1
♦ Naïve to disease-modifying therapies
♦ Natalizumab monotherapy for ~17 months with very good response
♦ Slowly progressive focal twitching and weakness of the left arm over a period of 2.5 months
♦ MRI: Subtle T2 hyperintensity in the pre-central gyrus that slowly progressed during this time
♦ First CSF negative, second CSF positive for JC virus
♦ Natalizumab discontinued and patient received 5 plasma exchanges♦ Natalizumab discontinued and patient received 5 plasma exchanges (PE) in 10 days, patient developed IRIS
♦ Current status: clinically stable and walking with assistance
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♦ Male 52 years, diagnosed 1992 in EU with Relapsing Remitting MS
PML in Post Marketing: Case 2y , g p g g
♦ 5-year history of azathioprine along with intervals of IFN
♦ Natalizumab monotherapy for approximately 14 months
♦ Left hemiparesis initially treated with steroids for presumed MS relapse
♦ S t hi h i l d d l ild iti h d♦ Symptoms, which included early mild cognitive changes, progressed over approximately 2 months, leading to hospitalization
♦ MRI: 2 large lesions atypical of MS predominantly in white matter, minimal Gd enhancement
♦ CSF positive for JC virus
♦ Natalizumab discontinued and the patient started plasma exchange and immunoadsorption, patient developed IRIS
♦ Current status: clinically stable, hospitalized
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PML in Post Marketing: Case 3♦ Female 59 years, diagnosed with MS in 2001♦ Multi-year history of treatment with β-interferons, glatiramer acetate,
and methotrexate♦ Natalizumab monotherapy for approximately 14 months♦ Initial symptoms included subjective memory problems, fatigue, hot
flashes (consistent with previous MS flares), speech deterioration, and worsening gaitworsening gait
♦ Progressed to expressive aphasia, slurred speech, worsened memory problems, some numbness in the legs, subjective gait problems
♦ MRI showed multiple non-enhancing lesions, consistent with a diagnosis of PML and the CSF tested positive for JC virus
P ti t d t l h d t t t ith fl i♦ Patient underwent plasma exchange and treatment with mefloquine, an experimental treatment option for PML
♦ Current status: clinically stable, under care of treating physician
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♦ Male 37 years, diagnosed 2006 in EU with aggressive MS
Overview of recent PML cases
– Naïve to disease-modifying therapies began natalizumab monotherapy for ~17 months
– Symptoms: slowly progressive focal twitching/weakness of left arm over ~ 2.5 months, MRI: subtle T2 hyperintensity in the pre-central gyrus that slowly progressed, CSF: 1st CSF - for JCV, 2nd +
– Natalizumab d/c, patient received 5 plasma exchanges (PE) in 10 days, developed IRIS, clinically stable and walking with assistance
♦ Male 52 years, diagnosed 1992 in EU with relapsing remitting MS
– 5-year Hx of azathioprine and β−IFNs, natalizumab monotherapy for ~14 months
– Symptoms: Left hemiparesis initially treated with steroids for presumed MS relapse early mild cognitive changes, progressed over ~ 2 months, leading to hospitalization, MRI: 2 large lesions atypical of MS predominantly in white matter, minimal Gd enhancement, CSF: + for JCV
– Natalizumab d/c, started PE, immunoadsorption, developed IRIS, clinically stable, hospitalized
♦ Female 59 years, diagnosed with MS in 2001– Multi-year Hx β-IFNs glatiramer acetate & methotrexate natalizumab monotherapy for ~14 monthsMulti year Hx β IFNs, glatiramer acetate, & methotrexate, natalizumab monotherapy for 14 months– Symptoms: initial symptoms included subjective memory problems, fatigue, hot flashes (consistent
with previous MS flares), speech deterioration, and worsening gait, progressed to expressive aphasia, slurred speech, worsened memory problems, some numbness in the legs, subjective gait problems, MRI: multiple non-enhancing lesions consistent with PML, CSF: + for JCV
– Natalizumab d/c, PE and Tx with mefloquine, clinically stable, under care of treating physician
19Triad for Monitoring and Diagnosis of PML
ClinicalClinicalVigilanceVigilanceClinicalClinical
VigilanceVigilance
MRIMRIAssessmentAssessment
MRIMRIAssessmentAssessment
CSFCSFAssessmentAssessment
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Algorithm for Diagnosis of PML♦ Clinical vigilance most important method of monitoring for PML♦ Clinical vigilance most important method of monitoring for PML
– Withhold natalizumab until PML can be excluded– A thorough neurological assessment should be performed at first
presentation of new/worsening clinical signs/symptoms
♦ If neurological assessment cannot rule out PML, a cranial MRI scan with contrast should be performed– MRI scan should be compared with previous MRI scan(s), if available– MRI alone can not exclude PML; repeat if clinical suspicion remains
♦ If clinical symptoms or MRI lesions remain suspicious for PML, CSF t ti f JCV b PCR h ld b d t dCSF testing for JCV by PCR should be conducted– In early PML, CSF can be negative for JCV DNA despite clinical and
radiographic findings– If JCV not detected, repeat test if clinical suspicion remains
BES3
Slide 20
BES3 Can this algorithm be shown as a diagram instead?Bruce E. Sands, 11/14/2008
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Immune Reconstitution Syndrome (IRS) or Immune Reconstitution Inflammatory Syndrome (IRIS)
♦ Condition seen in some AIDS or immunosuppression cases– Characterized by initial immune system recovery, followed by an
overwhelming inflammatory response to the previously acquired opportunistic infection, that paradoxically may make the symptoms of the initial infection worse
♦ If the CD4 count rapidly increases (due to effective treatment p y (of HIV or removal of other causes of immunosuppression), a sudden increase in the inflammatory response may produce a worsening of damage to the infected tissue
♦ Though IRIS can be potentially dangerous, it may also be indicative of potential long-term recovery from theindicative of potential long-term recovery from the opportunistic infection
Shelburne SA, et al. (2005) Incidence and risk factors for immune reconstitution inflammatory syndrome during highly active antiretroviral therapy. AIDS 19, 399-406.
Murdoch DM, et al. (2007) Immune reconstitution inflammatory syndrome (IRIS): review of common infectious manifestations and treatment options. AIDS Research and Therapy 2007, 4:9
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Plasma Exchange: Background♦ Immune reconstitution improves outcomes in
1 2immunosuppressed patients who develop PML1,2
♦ Plasma exchange is an established method for removal of large molecules from the peripheral circulation3
♦ Plasma exchange may lead to immune reconstitution and i i i th t f PML b l timay improve prognosis in the event of PML by accelerating
removal of natalizumab from the peripheral circulation
1Shitrit D, et al. Transpl Int 2005;11:658-665; 2Clifford DB, et al. Neurology. 1999;52:623-625; 3Khatri BO, et al. Neurology. 1985;35:312-319.
23Model Simulation of 5 Plasma Exchange
Sessions90% CI, α4-integrin receptor binding90% CI, natalizumab concentrations90% CI, natalizumab concentrationsMean α4-integrin receptor bindingMean natalizumab concentrations<1 μg/mL
atio
n (μ
g/m
L)
110120130140150
Final natalizumab infusion
PLEX sessions
α4-Inte90
100
110
120
Nat
aliz
umab
Con
cent
ra
30405060708090
100
grin Receptor B
inding (%
30
40
50
60
70
80
Plas
ma
0102030
Time (Days)
0 7 14 21 28
%)
0
10
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Bhupendra O. Khatri et al. Presentation #S22.005. 60th Annual Meeting of the American Academy of Neurology (16 April 2008).
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Plasma Exchange: Conclusions♦ Plasma exchange was effective at accelerating the normal
d li f t li b t ti ti i lldecline of serum natalizumab concentration over time in all patients
♦ Decreases in serum natalizumab concentrations to undetectable or very low levels (<1 μg/mL) resulted in subsequent decreases in α4-integrin receptor saturation
♦ In a pilot study in MS patients receiving natalizumab– Plasma exchange was generally well tolerated– There were no study discontinuations due to adverse events– All patients resumed scheduled infusions of natalizumab as part of
their MS therapytheir MS therapy
♦ Plasma exchange may be a suitable technique for rapidly removing natalizumab from the peripheral circulation in rare, but clinically appropriate, situations
Bhupendra O. Khatri et al. Presentation #S22.005. 60th Annual Meeting of the American Academy of Neurology (16 April 2008).
25CD INFORM: INVESTIGATING NATALIZUMAB THROUGH FURTHER
OBSERVATIONAL RESEARCH AND MONITORING
♦ FDA Post-Approval Commitment: 5 year observational pp ystudy of 2000 CD patients treated with natalizumab– Initiated in June 2008
♦ Objectives1° Determine the incidence and pattern of serious and/or clinically– 1 - Determine the incidence and pattern of serious and/or clinically significant infections, malignancies, and other serious adverse events (SAEs) in patients with CD treated with natalizumab
– 2 ° - Evaluate disease severity over time in CD patients treated with natalizumab based on changes in the Harvey-Bradshaw Index (HBI)
♦ Other data collected include– JC Viral DNA, or other laboratory testing for opportunistic infections
– ImmunKNOW assay on a subset of patients to assess the state of their immune function
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TYGRISTYSABRI Global Observation Program in Safety
♦ Global observational study to evaluate the long-term safety of natalizumab in a clinical practice setting in MS– Largest long-term safety study of any MS therapy ever conducted
♦ Expected enrollment: ~5000 patients with MS worldwide
♦ Patients evaluated at baseline and every 6 months for 5 yrsy y
♦ Information collected– Medical / MS history
– Prior use of immunomodulatory, antineoplastic, or immunosuppressive agents
– All serious adverse events (SAEs), including PML and other serious opportunistic infections (OIs), and malignancies
27Pregnancy Registry:
Background and Methods♦ A patient registry to evaluate the outcomes of pregnancy in
women with CD or MS exposed to natalizumab– Pregnant women who were exposed to natalizumab at any time
during the 3 months before conception or during pregnancy
– Pregnancies where the outcome is unknown (prospective reports)
Pregnancy reports where the outcome is known (retrospective– Pregnancy reports where the outcome is known (retrospective reports) will be collected and analyzed separately
♦ The following information will be collected within 4 weeks of the estimated date of delivery– Pregnancy outcome
– Infant characteristics (gestational age, gender, weight, length, Apgar scores, and birth order for multiple births)
– Description or attribution of any birth defect